The FAM104 proteins VCF1/2 promote the nuclear localization of p97/VCP

Author:

Körner Maria1,Meyer Susanne R1,Marincola Gabriella1ORCID,Kern Maximilian J2,Grimm Clemens1,Schuelein-Voelk Christina3,Fischer Utz1ORCID,Hofmann Kay4ORCID,Buchberger Alexander1ORCID

Affiliation:

1. University of Würzburg, Biocenter, Chair of Biochemistry I

2. Department of Molecular Cell Biology, Max Planck Institute of Biochemistry

3. Core Unit High-Content Microscopy, Biocenter, University of Würzburg

4. Institute of Genetics, University of Cologne

Abstract

The ATPase p97 (also known as VCP, Cdc48) has crucial functions in a variety of important cellular processes such as protein quality control, organellar homeostasis, and DNA damage repair, and its de-regulation is linked to neuromuscular diseases and cancer. p97 is tightly controlled by numerous regulatory cofactors, but the full range and function of the p97–cofactor network is unknown. Here, we identify the hitherto uncharacterized FAM104 proteins as a conserved family of p97 interactors. The two human family members VCP nuclear cofactor family member 1 and 2 (VCF1/2) bind p97 directly via a novel, alpha-helical motif and associate with p97-UFD1-NPL4 and p97-UBXN2B complexes in cells. VCF1/2 localize to the nucleus and promote the nuclear import of p97. Loss of VCF1/2 results in reduced nuclear p97 levels, slow growth, and hypersensitivity to chemical inhibition of p97 in the absence and presence of DNA damage, suggesting that FAM104 proteins are critical regulators of nuclear p97 functions.

Funder

German Research Foundation

Publisher

eLife Sciences Publications, Ltd

Subject

General Immunology and Microbiology,General Biochemistry, Genetics and Molecular Biology,General Medicine,General Neuroscience

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